Acute Decompensated Heart Failure : What is New ?
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Transcript of Acute Decompensated Heart Failure : What is New ?
Prof. U. C. SAMALMD, FICC, FACC, FIACM, FIAE, FISE, FISC, FAPVSEx-HOD Medicine & Prof. Cardiology Patna Medical College, Patna, BiharPast President, Indian College of CardiologyPermanent & Chief Trustee, ICC-HFFINational Executive Member, Cardiological Society of IndiaPresident, CSI Bihar
Acute Decompensated Heart Failure : What Is New ?
The best physician for a patient with HF would be one with excellent training, extensive experience, and superb judgment with regards to all aspects of the disease
He or she would not necessarily follow guidelines slavishly
Management for Heart Failure : Summary
J N Cohn Cir Heart Fail 1 87-88
• diuretics• ultrafiltration
Vasodilators • nitroglycerin• nesiritide• nitroprusside
INOTROPES • dobutamine• dopamine• levosimendan• nitroprusside
Fluid retention or redistribution ?
“dry out” “warm up & “dry out”
Assessment of hemodynamic profile : therapeutic implications
Adapted from Stevenson L W, Eur Heart j
HF Management: Principal changes from the 2008 guidelines
o An expansion of the indication for mineralocorticoid receptor antagonists (MRAs)
o A new indication for the sinus node inhibitor Ivabradine
o An expanded indication for cardiac resynchronisation therapy (CRT)
o New information on the role of coronary revascularisation in HF (PCI / CABG)
o Recognition of the growing use of ventricular assist devices (LVAD)
o The emergence of transcatheter valve interventionsESC guidelines for the diagnosis and treatment of acute and chronic heart failure
2012
Linking Short- term intervention with long-term benefit:What is needed?
Better understanding of Acute Heart Failure pathophysiology
ESC guidelines for the diagnosis and treatment of acute and chronic heart failure 2012 Reviewed by Ponikowski
Initial, short-term therapies [hours-days]Target Traditional
therapeutic approach
Effects on long-term outcome
Alleviate Congestion i.v. Diuretics ?May be detrimental
Reduce ↑ LV filling pressure
i.v. nitrates ?Potentially favourable
Hypoperfusion poor cardiac performance
i.v. inotropes Detrimental
Dissociation between symptomatic improvement, clinical stabilisation & favourable long-term outcome
Modified From Pang P S et al Eur Heart J 2010 31.784 -93
Primary outcome : Mortality Standard Oxygen Therapy
VersusNon Invasive Ventilation
Non-invasive ventilation [eg CPAP] should be considered in dyspnoeic patients with pulmonary oedema and a respiratory rate > 20 breaths / min to improve breathlessness and reduce hypercapnia and acidosis.
Non-invasive ventilation can reduce blood pressure and should not generally be used in pts with a SBP <85mmHg [ and BP should be monitored regularly when this treatment is used ] [class IIa, level B]
3 CPO Study
ESC guidelines for the diagnosis and treatment of acute and chronic heart failure 2012
Multiple reflections of ultrasound beams
ultrasound beams
ultrasound beams
Comet-tails echographic
imageNormal
echographic image horizontal
lines
Regular intervalReverberations
Transducer Transducer
Edematous Interlobular Septa
Normal Interlobular Septa
Ultrasound Comet-Tail Images: A Marker Of Pulmonary Edema
A: Typical comet-tail artifacts: hyperechogenic, coherent vertical bundles with narrow basis spreading from the transducer to the further border of the screen. This artifact is composed of multiple microreflections of the ultrasound beam.
A B
B: Normal subject, with regular, parallel, roughly horizontal hyperechogenic lines due to the lung-wall interface.
Chest. 2005;127(5):1690-1695. doi:10.1378/chest.127.5.1690
The four chest areas per side considered for complete eight zone lung ultrasound examination. These areas are used to evaluate for the presence of interstitial syndrome. Areas 1 and 2 denote the upper anterior and lower anterior chest areas, respectively. Areas 3 and 4 denote the upper lateral and basal lateral chest areas respectively.
HF: Monitoring to predict/ prevent ADHF admissions
• Devices: Externally applied Impedance Cardiography (PREDICT study 211 pts)
• Internally placed devices measuring intra thoracic impedance(PARTNER 2HF: CRT device with Impedance monitoring): predicted subsequent admission for ADHF
• PA / LA/ LVEDP monitoring devicesUsefulness uncertain for mortality benefit
Heart Failure Risk ScoresCirc HF 2013
End point: Death/ transplant/ Assist device• Heart Failure Survival Score(200pts):
– IHD, QRS>120ms, LVEF, Resting HR, mean BP, O2 consumption, ser Na
• Seattle Heart Failure model: (1100pts)– Age, LVEF, NYHA class, SBP, Diuretic dose,
Na+, uric acid, ser. Chol., lymph. count
- Sex, IHD, QRS >120ms, ICD, CRT, betablockers, ACEI, Statins, Allopurinol,
Heart Failure Risk Scores
• SHOCKED predictor: (900pts): Age>75, NYHA>II, AF, COPD, CKD, LVEF<20%, DM
• PACE: (900 pts) PVD, Age >70, Creatinine >2, EF < 20%,
• ADHERE registry( for acute mortality): SBP, Ser creatinine and BUN
• Frankenstein: BNP , 6′WT
In multivariable models, nearly all tested covariates performed similarly across LVEF strata for the outcome of death from any cause, as well as for HF-related and all-cause hospitalizations.Conclusions—We found that in a large, diverse contemporary HF population, risk assessment was strikingly similar across all LVEF categories. These data suggest that, although many HF therapies are uniquely applied to patients with reducedLVEF, individual prognostic factor performance does not seem to be significantly related to level of left ventricular systolic function. (Circ Heart Fail. 2013;6:635-646.)
Post Discharge Multi disciplinary Management Program
• Cardiac Rehabilitation: periodic follow up, education, optimize drug treatment, general medical care, exercise program, ensure access to hospital care
• Palliative Care: frequent hospitalization, not listed fro transplant or mechanical circulatory support, poor quality of life, dependence for daily needs, close to end of life
• Heart failure team: practitioner, nurse, pharmacist, dietician, psychologist, physiotherapist
Conclusion
• Acute Heart Failure, is a medical emergency and rapid, coordinated multi disciplinary approach can significantly reduce mortality.
• Stabilized patients of AHF, to have GDMT/ devices/ revascularization as indicated
• At discharge: patient education, counseling, compliance with GDMT and frequent clinic visits can prevent re-hospitalization for AHF
Proposed classification for patients who present with acute heart failure syndromesACCF/AHA
stageExplanation of stage
Worsening chronic HF (75%)
Stage C C: structural heart disease with prior or current symptoms of HF
Advanced HF (5%)
Stage D D: refractory HF requiring specialized interventions
De novo HF (20%)
Stage B most common, but also Stage A
Also neither A nor B
B: structural heart disease but without signs or symptoms of HF
A: at high risk for HF but without structural heart disease or symptoms of HF
Phases of acute heart failure syndromes managementPHASES
PHASES GOALS AVAILABLE TOOLS
Initial or emergencydepartment
phase ofmanagement
Treat life threatening conditions
Establish the diagnosis
Determine the clinical profile
Identify and treat precipitant
Disposition
Examples: STEMI - reperfusion therapy
History, physical exam, EKG, X-ray, natriuretic peptide level
BP, HR, signs (e.g. pulmonary oedema), ECG, X-ray,laboratory analysis, echocardiography
History, physical exam, X-ray, ECG, laboratory analysis
No universally accepted risk-stratification method
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
Phases of acute heart failure syndromes managementPHASES
PHASES GOALS AVAILABLE TOOLS
IN – HOSPITAL PHASE
Monitoring and reassessment
Assess right and left ventricular pressures
Assess and treat (in the right patient) other cardiac and non-cardiac conditions
Assess for myocardial viability
Signs/symptoms, HR, SBP, ECG, orthostatic changes, body weight, laboratory analysis (BUN/Cr, electrolytes), potentially BNP
SBP (orthostatic changes, valsalva manoeuvre), echocardiography, BNP/NT-proBNP, PA catheter
Echo-Doppler, cardiac catheterization, electrophysiology testing
MRI, stress testing, echocardiography, radionuclear studies
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
Phases of acute heart failure syndromes managementPHASES
PHASES GOALS AVAILABLE TOOLS
DISCHARGE PHASE
Assess functional capacity
Re-evaluate exacerbating factors (e.g. non-adherance, infection, anaemia, arrhythmias, hypertension) and treat accordingly
Optimize pharmacological therapy
Establish post-discharge planning
6 min walk test
Examples: physical therapy, education for diet control and medication, evaluation for sleep apnoea
ACCF/AHA and ESC guidelines
Discharge instructions including body weight monitoring, smoking cessation, medication adherance, follow-up
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
Drug failures in acute heart failureTrial name Drug tested Patients enrolledVMAC Nesiritide Decompensated CHF
Excluded SBP < 90 mmHg, Mean SBP > 124 mmHgNo LVEF cut point
OPTIME Milrinone Decompensated systolic heart failure, not requiring inotropesExcluded SBP < 80 mmHg, Mean SBP = 120 mmHgMean LVEF = 23%
VERITAS Tezosentan Acute heart failureTwo out of four-↑BNP, pulmonary oedema, CXR congestion,LVEF < 40%, Mean LVEF = 20% in VERITAS I and28% in VERITAS IIMean SBP = 131 in VERITAS I and 132 in VERITAS II
SURVIVE Levosimendan Acute decompensated HF requiring inotropesLVEF < 30%, Mean LVEF = 24$Mean SBP-116 mmHg
Trial name Drug tested Patients enrolledREVIVE -2 Levosimendan Acute decompensated HF
Symptomatic despite i.v. diureticLVEF < 35%, Excluded SBP > 90 mmHg
EVEREST Tolvaptan Hospitalized for decompensated CHFLVEF ≤ 40%, Excluded SBP < 120 mmHgMean LVEF = 27.5%, Mean SBP= 120 mmHg
PROTECT Iand II
Rolofylline Acute heart failure, Impaired renal function↑BNP
ASCEND-HF Nesiritide Acute decompensated heart failure
Drug failures in acute heart failure
Some new therapeutic agents for acute heartfailure and their potential targets
Agent For patients with theseclinical features
Diuretics, vasopressin antagonists,adenosine antagonists
Patients with signs of fluidoverload, high BNP
Vasodilators Normal to high SBP, high BNP
Inotropes Low SBP, signs ofHypoperfusion
Renal preservation agents Renal dysfunction
Myocardial protection agents CAD, or ongoing ischaemia
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
ESC divides pts. Into six clinical profiles1.Worsening or decompensated chronic HF2.Pulmonary Oedema3.Hypertensive HF4.Cardiogenic shock5.Isolated right HF6.ACS and HF with the explicit acknowledgement that there is overlap between groups
The ACCF/AHA divides patients based on presenting clinical profile into three main
groups: (i) volume overload, manifested by pulmonary and/or systemic congestion, usually due to increases in blood pressure (BP),(ii) severely reduced cardiac output often with hypotension, and(iii) combined volume overload and cardiogenic shock
ESC Guidelines
Initial Therapeutic Management Target Therapeutic example Mechanism of action Side effects
Alleviate congestion
IV furosemide Water and sodium excretion
Electrolyte abnormalities
Reduce elevated LV filling pressures
IV nitrates Direct relaxation of vascular smooth muscle cells through various mechanisms
Hypotension, decreased coronary perfusion pressure
Poor cardiac performance
Inotropes Activate camp or calcium sensitization resulting in improved contractility; also powerful vasodilators: in effect, inodilators
Hypotension, arrhythmias, myocardial damage, association with increased morbid events
Tachycardia and increased systemic blood pressure (i.e. in cases of excessive sympathetic tone
Beta-blockers: IV esmolol may be used when HF is related to AF with RVR and/or severe hypertension
Blockade of beta-1 and beta-2 receptors
Bradycardia,hypotension, negative inotropy; however given short half-life of esmolol, these side effects should be short lived
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
Short- and long-term novel therapies for AHF syndromesShort term Long term Both Levosimendan [LIDO, CASINO, SURVIVE] ? ?
Nesiritide[ROSE, DOSE-AHF]
Relaxin [RELAX-AHF]
Myosin Activators Omecamtiv Mecarbil [ATOMIC-AHF]
RyR2 stabilizers/ rycalsCinaciguat (UIT)Adenosine regulating agentsStresscopinIstaroxime [HORIZON-HF]Ularitide [TRUE-AHF, SIRIUS II, URGENT]
Urocrotins [UNICORN]
Hypertonic SalineUltrafiltration [RAPID-CHF, UNLOAD]
IABPEECP [PEECH]
CAFAIMT
Direct reninInhibitors (DRI)[ASTRONAUT]
MacronutrientsMicronutrientsCRT/AICD
Adenosine Antagonists[PROTECT, REACH UP rolofylline]
Vasopressin Antagonists [EVEREST, TACTICS-HF]
Digoxin [DIG]
CD-NP
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793 modified 2013
Clinical RELEVANCE of promising novel biomarkers(AHFS)Biomarker Diagnosis Prognosis Therapy guidance Cardiac
ProductionNT-proBNP and BNP
++++ ++++ ++ Solely
Serum Sodium ++ ++ ++ No
Serum Creatinine ++ ++ ++ No
MR-proANP +++ ++++ Likely similar to NT-ProBNP/BNP
Solely
sST2 + ++++ ? Not ExclusivelyHs troponin-I [EFFECT]
+ ++++ ? Solely
MR-proADM - ++++ ? No
Cystatin C - ++++ ? NoNGAL - ++++ ? NoGDF-15 - +++ ? Not Exclusively- Trace protein - +++ ? NoGal-3 - +++ ? Not exclusivelyCRP - ++ ? NoTNF- - ++ ? NoIL-6 - ++ ? NoPTX3 - ++ ? UnknownMPO - ++ ? Not exclusivelyET-1 - ++ ? Not exclusivelyCopeptin - ++ ? NoPCT ++ ++ ++ No
27
Clinical Chemistry 58:1 127–138 (2012)
Summary of the main utility biomarkers in AHFSBiomarkers Diagnosis & pathophysiology Adverse prognosis
Serum sodium n.v. 136-145mmol/LAHF –RAA activation
<120mmol/L
Serum creatinine n.v. 0.5 – 1.5mg/dLCardiorenal syndrome
> 150µmol/L
Serum uric acid n.V m 3.1 -8.1mg/100ml, 2.2 -7.1mg/100mlAHF –oxidative stress
>1.5mg/dl>9.8mg/dl
NPs [blood & serum]BNPNT-pro-BNPMR-pro-ANP
v.n. HF cut off<100pg/ml; >400pg/ml<400pg/ml; >2000pg/ml<120pmol/l; 120pmol/lAHF left ventricular volume and pressure overload [heart muscle stretching]
> 1000pg/ml> 5000pg/ml--
ST2 [serum] n.V 1.75 -34.3U/mlAHF overload
>10ng/ml
Summary of the main utility biomarkers in AHFS
Biomarkers Diagnosis & pathophysiology Adverse prognosis
PCT [serum] Cut off 0.05ng/ml 0.05 -0.5ng/ml local infection0.5-2ng/ml systemic infection2-10ng/ml SIRS – sepsis>10ng/ml sepsis
NGAL [serum and urine]
Cut off 150ng/ml serum, 130ng/ml urineCardiorenal syndrome
>100ng/ml
Copeptin [serum] Median 3.7pmol/lAHF vascular alterations
>54.2pmol/l
MR-proADM [SERUM] AHF vascular alterations >2.15nmol/l
ADMA AHF oxidative stress
Modes of presentation of ADHFClinical status Heart
rateSBP
mmHgCl L /
min /m3Pulmonary
capillary wedge
pressure mmHg
Congestion
killip/forrester
Diuresis Hypoperfusion
End organ hypoperfusion
I acute decompensated congestive heart failure
+ / - Low normal / high
Low normal / high
Mild elevation K II / F II + +/- _
II Acute heart failure with hypertension/ hypertensive crisis
Usually elevated
High +/- >18 K II-IV/ F II / III
+/- +/- + WITH CNS symptoms
III Acute heartfailure withpulmonary edema
+ Low normal
Low Elevated K III / F II + +/- -
IVa Cardiogenicshocka/low-outputsyndrome
+ Low normal
Low, <2.2 >16 K III-IV/ F I-III
Low + +
IVb Severecardiogenic shock
>90 <90 <1.8 >18 K IV / F IV Very low ++ +
V High-outputfailure
+ +/- + +/- K II / F I-II + - -
VI Right-sided acuteheart failure
Usually low
Low Low Low F I +/- +/-, acute onset
+/-
Patient presenting with dyspnea
Differential diagnosis cardiac -- Consider acute coronary syndrome
Physical exam, chest x-ray, ECG, BNP level
Treatment option for HF with SBP <90mmHg or shock –diuretics, inotropes, vasodilators and /or nesiritide to follow
BNP <100pg/ml BNP 100-500pg/ml BNP >500pg/ml
HF very unlikely [2%] Clinical suspicion of HF or past h/o HF
HF very likely [95%]
HF highly probable [90%]Differential diagnosis noncardiac -- consider COPD, pulmonary embolism, asthma, pneumonia, sepsis
Treatment option for HF with SBP > 90mmHg -- diuretics with nesritide esp. with CKD & pulmonary congestion may consider adding vasodilators if hypertensive may consdider adding inotropes for poor perfusion
Treatment option --•Diuretics as required •Consider nesritide if any of the following - Scr>1.5mg/dl, CrCl <60ml/min, BUN >10mg/dl, pulmonary congestion or for border line hemodynamic instability
Comprehensive Assessment
Potential targets Method of assessmentCongestion JVP, Body wt, peripheral edemaLV function, valvular ds, wall motion abnormalities, aneurysm
ECHO Doppler, MRI, Nuclear imaging
Ischaemia Pharmacological or exercise testing with imaging
CAD Cardiac catheterization and angiography
Ventricular dyssnchrony [wide QRS]
Electrocardiogram
Viable but dysfunctional myocardium
Low dose dobutamine ECHO, MRI
Myocardium Coronary arteries
Electrical system
Valves•Surgery•Procedural•Statins•Per EDC guidelines
Pericardium
LV dysfunction
•ACE-I or ARB•Beta blockers•Aldosterone antagonist•Hydral / ISDN•Digoxin•Macronutrients•Micronutrients•Metabolic modulators
CAD•Anti platelet•Statins•Revascularization•Other ESC guideline recommended therapy for secondary prevention
Sudden cardiac death
•ICD•B- blockers•Aldesterione antagonist
Ventriculasr dysschrony
•CRT +/- ICD
Atrial fibrillation•Rate control – digoxin – b- blocker, non dihydropyridine ca channel blockers•Warfarin•Rhythm control•MAZE procedure
Congestion – [ salt restriction, diuretics, ultrafiltarion, vasopressin antagonists]
Hypertension [ACE I or ARB, diuretics, other per ESC guidelines
Enhance adherence [education, disease management, performance improvement system
Cardiac reconstruction[five overacting thematic targets – myocardium, coronary arteries, electrical system, pericardium, valves]
0 10 20 30 40 50
right HF
hypertensive HF
cardiogenic shock
pulmonary edema
decompensated HF
De novo AH
ADCHF
all
Mortality %
Frontiers in Cardiovascular Medicine EHJ 2010:31;784-793
AHFS : NOT VERIFIEDSimilarities and differences between acute MI & AHFS in
hospitalization in the US
Incidence 1 million per year 1 million per yearMortality Pre hospitalization In hospital After discharge [ 60-90 d]
High3-4%2%
?3-4%10%
Myocardial injury Yes LikelyPathophysiological target Clearly defined
[coronary thrombosis]Uncertain
Clinical benefits of interventions in published clinical trial
Beneficial Minimal / no benefit or deleterious compared with placebo
ACC / AHA recommendation LEVEL A NONE
Acute Heart Failure Syndrome(s)
• Acute heart failure (AHF) is defined as a rapid onset or change in the signs and symptoms of HF, resulting in the need for urgent therapy.
• Symptoms are primarily the result of severe pulmonary congestion due to elevated left ventricular (LV) filling pressures (with or without low cardiac output).
• AHFS can occur in patients with preserved or reduced ejection fraction (EF).
• Concurrent cardiovascular conditions such as coronary heart disease (CHD), hypertension, valvular heart disease, atrial arrhythmias, and/or
noncardiac conditions (including renal dysfunction, diabetes, anemia) are often present and may precipitate or contribute to the pathophysiology of this syndrome
EBM in AHFS?• The first randomized placebo-controlled AHFS trials
were published as late as 2002.Cuffe MS, et al. for the Outcomes of a Prospective Trial of Intravenous Milrinone for Exacerbations of Chronic Heart Failure (OPTIME-CHF)
Investigators. Effects of short-term, intravenous milrinone on acute exacerbation of chronic heart failure: a randomized controlled trial. JAMA.
2002; 287: 1541–1547.
Publication Committee for the VMAC Investigators. Intravenous nesiritide vs nitroglycerin for treatment of decompensated congestive heart
failure: a randomized controlled trial. JAMA. 2002; 287: 1531–1540
• None of the placebo-controlled AHFS studies conducted to date has shown either a consistent improvement of in-hospital or postdischarge survival or a decrease in readmissions.
AHFS – Goals of treatment• † Emergency treatment phase• Improve symptoms• Restore oxygenation• Improve organ perfusion and haemodynamics• Limit cardiac/renal damage• Minimize ICU length of stay• † In-hospital management phase• Stabilize patient and optimize treatment strategy• Initiate appropriate (life-saving) pharmacological therapy• Consider device therapy in appropriate patients• Minimize hospital length of stay• † Discharge planning phase• Plan follow-up strategy• Educate and initiate appropriate lifestyle adjustments• Provide adequate secondary prophylaxis• Prevent early readmission• Improve quality of life and survival
AHFS: which appropriate targets of therapy ?
• Traditionally, reduction in pulmonary capillary wedge pressure (PCWP) and/or increase in cardiac output.
• However, other therapeutic targets may include blood pressure control, myocardial protection, neurohormonal modulation, and preservation of renal function.
Treatment of AHFS Patients
• The emergency treatment phase
Patient Selection and TreatmentCongestion at Rest
YesNo
Warm & DryPCWP normal
CI normal (compensated)
Cold & WetPCWP elevatedCI decreased
Cold & DryPCWP low/normal
CI decreased
VasodilatorsNitroprussideNitroglycerin
Inotropic DrugsDobutamine
MilrinoneCalcium Sensitizers
Normal SVR
High SVR
LowPerfusion
at Rest
No
Yes
Warm & WetPCWP elevated
CI normal
Natriuretic PeptideNesiritide or
Stevenson LW. Eur J Heart Fail. 1999;1:251.
Adverse Drug Effects• Non-Potassium-Sparing Diuretics
Intravenous loop diuretics may improve symptoms and fluid loss initially but also may contribute to renal function decline. This may be related not only to intravascular volume depletion but also to further neurohormonal activation resulting in a vasomotor nephropathy.
• Intravenous loop diuretics may be associated with worse outcomes in AHFS patients.
• Inotropic TherapyIntravenous inotropes increase myocardial oxygen consumption, causing myocardial damage in the setting of hibernating myocardium. Use of inotropes has consistently been associated with increased mortality.
• VasodilatorsExcessive vasodilatation in AHFS may lead to blood pressure decrease, potentially exacerbating myocardial ischemia and renal hypoperfusion.
AHFS: which appropriate targets of therapy ?Perspectives
• Managing fluids,
• Preserving renal function
Vaso active drugs in ADHFRelaxin: Serelaxin
• RELAX AHF:1160 pt. of ADHF with preserved SBP >115 mmHg.• Serelaxin 30 ug/kg/day x48 hrs or Placebo• Significant improvement in dyspnoea scale• No impact on short term mortality/ HF readmission at 60 days,
though 180 day mortality was significantly lower.• Hypotensive episodes higher but renal dysfunction less than
placebo group• No limitation: dobutamine milrinone (increase intercellular calcium
in myocytes leading to tachycardia and arrhythmias, levosimendon calcium sensitiser causes atrial and ventricular arrhythmias, and like milrinone may be limited by hypotension.
• FDA grants Breakthrough Therapy designation to Novartis' serelaxin (RLX030) for acute heart failure.
Biology of Relaxin and Potential Beneficial Effects in Heart Failure
Teichman SL, Unemori E, Teerlink JR, Cotter G, Metra M - Curr Heart Fail Rep (2010)
Endogenous peptide associated with pregnancy, and acts through relaxin receptor: reduce inflammation, decrease fibrosis, attenuate ventricular remodeling, increase vasodilation, promote renal blood flow, increase vascular endothelial growth factor, and angiogenesis.
↓Inflammation ↓Fibrosis ↑Vasodilation Renal effects Angiogenesis
Relaxin Receptor
RelaxinPregnancy associated endogenous peptide
Relaxin ReceptorRelaxin
Omecamtiv Mecarbil (OM) is a Novel Selective Cardiac Myosin Activator
Malik Fl, et al. Science 2011; 331:1439-43Teerlink JR, et al. Lancet 2011; 378:667-75; Cleland JGF, et al. Lancet 2011; 378:676-83
Mechanochemical Cycle of Myosin
• • Increases duration of systole• Increases stroke volume• No Increase in myocyte calcium• No change in dp/dtmax
• No increase in MVO2
ATOMIC-AHF Phase 2; 613 pts .X 48 hrs random IV dose 115; 230; 310 ng/ml.COSMIC-HF chronic oral therapy; oral alone or IV to oral transition.
Omecamtiv mecarbil increases the entry rate of myosin into the tightly-
bound, force-producing state with actin
“More hands pulling on the rope”
• Efficacy– OM did not meet the 1° endpoint of dyspnoea relief– Appeared to improve dyspnoea in Cohort 3– Trends towards reduction of worsening HF
• Safety– Overall SAE profile and tolerability similar to placebo– Increase in troponin; no clear relationship to OM concentration– Numerical imbalance in MIs in Cohort 3 – No evidence of pro-arrhythmia
• Pharmacology– PK similar to healthy volunteers and stable HF patients – Systolic ejection time significantly increased consistent with MOA– Small fall in heart rate & rise in systolic BP at higher doses
Summary
Though at present investigational the drug of the future in AHF Janccin B: New Heart failure inotrope could be ‘Holy Grail’. IMNG Medical Media September 5, 2013
John J. V. McMurray et al, on behalf of the ATOMIC-AHF Investigators and Patients
Levosimendan enhances contractility by increasing responsiveness of myofilaments to calcium. The cardiac myosin activator Omecamtiv mecarbil stimulates myosin adenosine triphosphatase (ATPase), thereby increasing force generation. Istaroxime inhibits activity of plasma membrane sodium-potassium ATPase and increases the activity of sarcoplasmic/endoplasmic reticulum calcium ATPase (SERCA).
Mechanism of action of novel contractility-enhancing medications.
Omecamtiv mecarbil
(Modified from Tavares M, Rezlan E, Vostroknoutova I, et al. New pharmacologic therapies for acute heart failure. Crit Care Med 2008; 36[Suppl]:S112-S120.)
• Istaroxime is a novel intravenous agent with inotropic and lusitropic properties related to inhibition of Na/K adenosine triphosphatase (ATPase) and stimulation of sarcoplasmic reticulum calcium ATPase.
• 120 AHF pts and reduced systolic function. Three sequential cohorts of 40 patients each were randomized 3:1 istaroxime:placebo to a continuous 6-h infusion. The first cohort received 0.5 g/kg/min, the second 1.0 g/kg/min, and the third 1.5 g/kg/min istaroxime or placebo.
• In patients hospitalized with HF, istaroxime improved PCWP and possibly diastolic function. In contrast to available inotropes, istaroxime increased SBP and decreased HR.
Istaroxime
Mihai Gheorghiade et al JACC 2008:03;015
Vaso active drugs in ADHFUlaritide
• Synthetic form of Urodilantin: human natriuretic peptide produced in kidney: induces natriuresis and diuresis. Also potent vasodilator( increases intracellular cyclic GMP) and increased renal blood flow) : Two double blind studies have shown favorable outcome in ADHF by symptom improvement and hemodynamics.
• Phase 3 trial(TRUE-AHF >2110 pts) - ongoing study.
Investigational drugs in ADHFAdenosine A1 receptor antagonist:
Rolofylline• Preserve GFR, improve diuresis, increase
sodium excretion by kidney• Phase 2 trial: better relief of dyspnoea and
lesser renal dysfunction• Phase 3 trial: PROTEC:2033 pts.:
negative trial with none of the primary end points significant and safety was questioned due to neurological side effects: seizure and stroke
• Small studies have indicated that adenosine A1 receptor antagonists enhance diuresis and may improve renal function in patients with chronic heart failure or AHF.
• 2,033 AHF pts, volume overload, eCrCl 20 - 80 ml/min, and elevated BNP randomized (2:1) within 24 h of hospital presentation to rolofylline 30 mg/day or intravenous placebo for up to 3 days.
• In this large, phase III clinical trial, the adenosine A1 receptor antagonist rolofylline did not prevent persistent worsening renal function in AHF patients with volume overload and renal dysfunction.
Rolofylline
•Effects of rolofylline on endpoints in relation to baseline renal function.
•The secondary morbidity/mortality endpoint, the risk of death or cardiovascular or renal rehospitalization through day 60, was lower in the rolofylline group compared with the placebo group only in patients with a baseline eCrCl 30 ml/min (hazard ratio: 0.64; 95% CI: 0.43 to 0.95), but not in the other subgroups
Rolofylline
• Loop diuretics are an essential component of therapy for patients with acute decompensated heart failure, but there are few prospective data to guide their use.
• In a prospective, double-blind, randomized trial, we assigned 308 patients with ADHF to receive furosemide administered intravenously by means of either a bolus every 12 hours or continuous infusion and at either a low dose (equivalent to the patient’s previous oral dose) or a high dose (2.5 times the previous oral dose).
• Among patients with ADHF, there were no significant differences in patients’ global assessment of symptoms or in the change in renal function when diuretic therapy was administered by bolus as compared with continuous infusion or at a high dose as compared with a low dose.
Furosemide
• The study tests the hypothesis that in patients admitted with acutely decompensated heart failure (ADHF), achievement of adequate body hydration status with intensive medical therapy, modulated by combined bioelectrical vectorial impedance analysis (BIVA) and B-type natriuretic peptide (BNP) measurement, may contribute to optimize the timing of patient’s discharge and to improve clinical outcomes.
• 300 ADHF pts underwent serial BIVA and BNP measurement. Therapy was titrated to reach a BNP value of \250 pg/ml, whenever possible.
• Our study confirms the hypothesis that combined BNP/BIVA sequential measurementshelp to achieve adequate fluid balance status in patients with ADHF and can be used to drive a ‘‘tailored therapy,’’ allowing clinicians to identify high-risk patients and possibly to reduce the incidence of complications secondary to fluid management strategies.
Ultrafiltration
AHFS: which appropriate targets of therapy ?
• Contractility
• Diastole
•Urocortins are a recently discovered group of peptide hormones of the corticotropin releasing factor family. They bind with a strong affinity to the CRH-R2 receptor, which is highly expressed in the myocardium and in the vascular endothelium.
•Urocortins exhibit potent inotropic and lusitropic effects on rat and sheep hearts and activates a group of myocyte protective pathways collectively known as ‘reperfusion injury salvage kinase’.
•In healthy humans show that brief intravenous infusions of urocortin 2 in healthy humans induce pronounced dose-related increases in cardiac output, heart rate, and left ventricular ejection fraction while decreasing systemic vascular resistance; similar effects were seen in HF patients.
Urocortins
AHFS: which appropriate targets of therapy ?
• Vasomotion
• Nesiritide is approved in the United States for early relief of dyspnea in patients with acute heart failure. Previous meta-analyses have raised questions regarding renal toxicity and the mortality associated with this agent.
• We randomly assigned 7141 patients
• Coprimary end points were the change in dyspnea at 6 and 24 hours, and the composite end point of rehospitalization for heart failure or death within 30 days.
• Nesiritide was not associated with an increase or a decrease in the rate of death and rehospitalization and had a small, nonsignificant effect on dyspnea when used in combination with other therapies.
• It was not associated with a worsening of renal function, but it was associated with an increase in rates of hypotension. On the basis of these results, nesiritide cannot be recommended for routine use in the broad population of patients with acute heart failure.
Nesiritide
These molecules have been engineered to combine the beneficial aspects of different natriuretic peptides into a single molecule while minimizing potentially negative actions.
CD-NP is a combination of C-type natriuretic peptide (CNP) and Dendroapsis NP(DNP).
Although lacking natriuretic effects, CNP is a more selective venodilator than BNP, thus reducing the risk of significant hypotension. On the other side, DNP possesses significant natriuretic activity, at the expense of possible hypotensive effects.
The chimeric peptide CD-NP combines the favourable natriuretic effects of DNP with the venodilatory profile of CNP, reducing the risk for harmful side effects.
Preliminary studies in AHFS patients are ongoing.
Chimeric natriuretic peptides
• Cinaciguat (BAY 58-2667) is a soluble guanylate cyclase (sGC, second messenger that internalizes the message carried by intercellular messengers such as peptide hormones and NO) activator that is being developed as a first-in-class treatment for acute decompensated heart failure (ADHF). It acts independently of the sGC ligand nitric oxide.
• Cardioprotective effects in animal models, and pilot clinical studies found that it was well tolerated, unloaded the heart and increased cardiac output.
• This placebo-controlled, randomized, double-blind, multicenter, international phase IIb study investigated the safety and efficacy of intravenous cinaciguat (per-protocol) as add-on to standard therapy in 139 patients with ADHF (NYHA functional class III and IV; pulmonary capillary wedge pressure [PCWP] ≥ 18 mmHg).
• Cinaciguat rapidly and significantly reduced PCWP and PVR and increased cardiac output in patients with ADHF, without impairing cardiac or renal function. Hypotension occurred in some patients; further dose titration studies are therefore required to establish the optimal dosing strategy for this promising new therapy.
Cinaciguat
JACC Mar 9,2010 Vol:55 issue 10A
Adenosine regulating agents
•This new class of drugs, whose prototype is represented by acadesine, has been developed to mimic the protective effects of adenosine during ischaemia.
•Acadesine exerts its pharmacological actions by increasing adenosine bioavailability and by activating 50adenosine monophosphate (AMP) signalling cascade via its metabolite 5-aminoimidazole-4-carboxamide riboside (ZMP).
•The first mechanism leads to multiple anti-ischaemic effects (maintenance of endothelial function and vasodilation, inhibition of platelet aggregation and neutrophil activation), whereas the latter ameliorates glucose uptake and free fatty acid oxidation thus increasing ATP synthesis. Importantly, acadesine exerts its actions only in areas undergoing net ATP catabolism (such as ischaemic tissues) thereby avoiding potentially harmful peripheral vasodilator effects.
Acadesine
StresscopinHuman stresscopin is a corticotropin-releasing factor type 2 receptor selective agonist and a member of the CRF peptide family. Stimulation of CRFR2 improves cardiac output and LVEF.
62 pts with HF and LVEF ≤ 35% were instrumented with a pulmonary artery catheter and randomly assigned (ratio 3:1) to receive an intravenous infusion of stresscopin or placebo. The main study was an ascending dose study of three doses (5, 15, and 30 ng/kg/min) of study drug or placebo administered in sequential 1 h intervals (3 h total). Statistically significant increases in CI and reduction in SVR were observed with both the 15 ng/kg/min (2 h time point) and 30 ng/kg/min (3 h time point) doses of stresscopin without significant changes in HR or SBP. No statistically significant reductions in PCWP were seen with any dose tested in the primary analysis, although a trend towards reduction was seen.
In HF patients with reduced LVEF and CI, ascending doses of stresscopin were associated with progressive increases in CI and reductions in SVR without significant effects on PCWP, HR, or SBP.
In-Hospital Management Phase
• This phase begins once the patient is stabilized and dyspnea is improved.
• Because a significant number of patients continue to have signs and symptoms of HF, the goals of this phase are continued hemodynamic and symptomatic improvement while preventing myocardial and renal injury.
• Patients who are not treated with ACE inhibitors, angiotensin receptor blockers, ß-blockers, or aldosterone antagonists should receive these therapies, as
recommended by recent guidelines
AHFS: in-hospital management (ADHERE/OPTIMIZE-CHF/EURO-HF)
Discharge-Planning Phase
• Despite the clinical evidence supporting the use of implantable cardiac defibrillators and cardiac resynchronization therapy in patients with chronic HF and systolic dysfunction, their role in AHFS patients is not clear.
• The available data suggest that a significant number of AHFS patients are not being evaluated for potential beneficial surgical procedures that include myocardial revascularization, LV reconstruction,
mitral valve surgery, or cardiac transplantation.
AHFS where are we? Where are we going?• AHFS is a complex condition with substantial morbidity and
mortality and enormous utilization of health resources and cost.
• There are numerous challenges in caring for this population. • Uniform AHFS classification is currently lacking, and management
strategies vary markedly.
• There is a general consensus that to reduce mortality, morbidity, and the economic burden of AHFS, systematic research efforts on clinical application and translation of promising basic science results are needed.
• Pathophysiologically based interventions (eg, cardiorenal syndrome) may be particularly appealing.
• A special focus should be on choice of appropriate management strategies, including minimizing the use of drugs with adverse effects and development and validation of known prognostic markers to guide AHFS interventions.
…of note, every large published clinical trial conducted in patients with AHFs has been negative in terms of efficacy, safety, or both.
…However, most international multicenter clinical trials completed to date were conducted on fairly undifferentiated populations of patients with AHFs.
….homogeneous pathophysiological disease states within the heterogeneity of aHFs is of paramount importance to clinical trial design and aHFs therapy.
… Future trials conducted in aHFs must abandon the ‘one-sizefits- all’ approach in favor of an approach that takes into account the varied and distinct pathophysiologies of aHFs.
Milton Packer 2008 JCF
• … Yet, despite substantial advances in our understanding and management of heart failure, we have had
• few successes and many failures.
• Nearly 1,000 new drugs and devices have been developed for the treatment of heart failure duringthe past 20 years, but only 9 have received regulatory approval and are being used in the clinical setting.
• Most of our efforts to correct fluid retention, stimulate the inotropic state of the heart, and modulate neurohormonal systems have not predictably improved the condition of patients with HF…
Apelin
rhBNP
DR I
MKRG
S SS
SGLG
FC CS SG
SGQVMK V L R
RH
KPS
Effects of NesiritideVenous, arterial, coronary
VASODILATION
CARDIACINDEX
PreloadAfterloadPCWPDyspnea
HEMODYNAMIC
CARDIAC No increase in HRNot proarrhythmic
AldosteroneEndothelinNorepinephrine
SYMPATHETIC AND NEUROHORMONAL SYSTEMS
Fluid volumePreloadDiuretic usage
NATRIURESISDIURESIS
RENAL
Risk Scores to Predict Outcomes in HF
Risk Score Reference (from full-text guideline)/Link Chronic HFAll patients with chronic HFSeattle Heart Failure Model (204) / http://SeattleHeartFailureModel.org
Heart Failure Survival Score (200) / http://handheld.softpedia.com/get/Health/Calculator/HFSS-Calc-37354.shtml
CHARM Risk Score (207) CORONA Risk Score (208)Specific to chronic HFpEFI-PRESERVE Score (202)
Acutely Decompensated HF
ADHERE Classification and Regression Tree (CART) Model
(201)
American Heart Association Get With the Guidelines Score
(206) / http://www.heart.org/HEARTORG/HealthcareProfessional/GetWithTheGuidelinesHFStroke/GetWithTheGuidelinesHeartFailureHomePage/Get-With-The-Guidelines-Heart-Failure-Home- %20Page_UCM_306087_SubHomePage.jsp
EFFECT Risk Score (203) / http://www.ccort.ca/Research/CHFRiskModel.aspx
ESCAPE Risk Model and Discharge Score (215)
OPTIMIZE HF Risk-Prediction Nomogram (216)
Diuretics in Hospitalized Patients
Patients with HF admitted with evidence of significant fluid overload should be promptly treated with intravenous loop diuretics to reduce morbidity.
If patients are already receiving loop diuretic therapy, the initial intravenous dose should equal or exceed their chronic oral daily dose and should be given as either intermittent boluses or continuous infusion. Urine output and signs and symptoms of congestion should be serially assessed, and the diuretic dose should be adjusted accordingly to relieve symptoms, reduce volume excess, and avoid hypotension.
I IIaIIb III
I IIaIIb III
Diuretics in Hospitalized Patients (cont.)
The effect of HF treatment should be monitored with careful measurement of fluid intake and output, vital signs, body weight that is determined at the same time each day, and clinical signs and symptoms of systemic perfusion and congestion. Daily serum electrolytes, urea nitrogen, and creatinine concentrations should be measured during the use of intravenous diuretics or active titration of HF medications.
When diuresis is inadequate to relieve symptoms, it is reasonable to intensify the diuretic regimen using either:
a. higher doses of intravenous loop diuretics.b. addition of a second (e.g., thiazide) diuretic.
I IIaIIb III
I IIa IIb III
Diuretics in Hospitalized Patients (cont.)
Low-dose dopamine infusion may be considered in addition to loop diuretic therapy to improve diuresis and better preserve renal function and renal blood flow.
I IIa IIb III
Renal Replacement Therapy
The Hospitalized Patient
Renal Replacement Therapy
Ultrafiltration may be considered for patients with obvious volume overload to alleviate congestive symptoms and fluid weight.
Ultrafiltration may be considered for patients with refractory congestion not responding to medical therapy.
I IIaIIb III
I IIa IIb III
Parenteral Therapy in Hospitalized HF
If symptomatic hypotension is absent, intravenous nitroglycerin, nitroprusside or nesiritide may be considered an adjuvant to diuretic therapy for relief of dyspnea in patients admitted with acutely decompensated HF.
I IIaIIb III
Arginine Vasopressin Antagonists
In patients hospitalized with volume overload, including HF, who have persistent severe hyponatremia and are at risk for or having active cognitive symptoms despite water restriction and maximization of GDMT, vasopressin antagonists may be considered in the short term to improve serum sodium concentration in hypervolemic, hyponatremic states with either a V2 receptor selective or a nonselective vasopressin antagonist.
I IIa IIb III
Arginine Vasopressin Antagonists
• Risk of liver injury has been described in those with pre-existing liver disease when exposed to AVP antagonists
• http://www.fda.gov/Safety/MedWatch/SafetyInformation/SafetyAlertsforHumanMedicalProducts/ucm336669.htm - accessed 06/04/13
Surgical/Percutaneous/Transcatheter Interventional
Treatment of HFCoronary artery revascularization via CABG or percutaneous intervention is indicated for patients (HFpEF and HFrEF) on GDMT with angina and suitable coronary anatomy, especially for a left main stenosis (>50%) or left main equivalent disease.
CABG to improve survival is reasonable in patients with mild to moderate LV systolic dysfunction (EF 35% to 50%) and significant (≥70% diameter stenosis) multivessel CAD or proximal LAD coronary artery stenosis when viable myocardium is present in the region of intended revascularization.
I IIa IIb III
I IIaIIb III
Surgical/Percutaneous/Transcatheter Interventional
Treatment of HF (cont.)CABG or medical therapy is reasonable to improve morbidity and cardiovascular mortality for patients with severe LV dysfunction (EF <35%), HF, and significant CAD.
Surgical aortic valve replacement is reasonable for patients with critical aortic stenosis and a predicted surgical mortality of no greater than 10%.
Transcatheter aortic valve replacement after careful candidate consideration is reasonable for patients with critical aortic stenosis who are deemed inoperable.
I IIaIIb III
I IIa IIb III
I IIa IIb III
Surgical/Percutaneous/Transcatheter Interventional
Treatment of HF (cont.)CABG may be considered with the intent of improving survival in patients with ischemic heart disease with severe LV systolic dysfunction (EF <35%), and operable coronary anatomy whether or not viable myocardium is present.
Transcatheter mitral valve repair or mitral valve surgery for functional mitral insufficiency is of uncertain benefit and should only be considered after careful candidate selection and with a background of GDMT.
Surgical reverse remodeling or LV aneurysmectomy may be considered in carefully selected patients with HFrEF for specific indications including intractable HF and ventricular arrhythmias.
I IIaIIb III
I IIaIIb III
I IIa IIb III
Cystatin C and NT-pro BNP
Furosemide and HTS• Theory:
– Offsets the counterproductive neurohormonal up-regulation
– transiently improves hemodynamics– promotes renal Na extraction with accompanied net
water loss and preservation of renal function
• Seems counterintuitive, but in a way, it is “giving the body the very sodium it is trying so hard to retain”
Liszowski, Curr Heart Fail Rep. 2010;7:134-39
Furosemide and Hypertonic Saline– ↑ natriuresis and diuresis– Results maintained over time , when continuing PO
diuretic therapy and low Na (but not restricted) diet– Better survival at 48 months (55 vs 13%)– Allows more rapid attainment of dry weight– Faster in BNP (↓ BNP maintained with higher Na diet)– Lower LOS and 30 day readmission rate.– Improvement in renal fn– No adverse cardiac events– US and Brazil w/ ongoing
large studies nowPaterna, et al. Eur. J Heart Fail 2000;2:305-13Paterna et al. Clin Drug Interact; 25:165-174Paterna et al.JACC 2005;45:1887-2003Licata et al. Am Heart J 2003;145;459-66
(1) Symptom relief.(2) Measures of congestion relief (i.e. improvement in clinical signs).(3) Index hospitalization data (e.g. length of stay).(4) Prevention of end-organ damage (heart and kidney).(5) Post-discharge: death and rehospitalization data.
Federal Drug Administration (FDA) Study Group as a generalguide for choosing the components of the endpoints to beincluded when testing different types of drugs in different patientsubgroups, although not all of them would be necessary in asingle trial
Position Statement European Journal of Heart Failure (2011)
Simplified schematic of guanylyl cyclase (GC) pathways, which have cyclic guanosine monophosphate (cGMP) as their second messenger. Nitric oxide is produced by endothelial cells and activates soluble GC in the target cell. ANP and BNP stimulate GC-A (also called NP receptor A), while CNP stimulates GC-B (also called NP receptor B). DNP is a GC-agonist first discovered in snake venom. CD-NP is a chimeric peptide composed of the ring structure and amino terminus of CNP and the carboxyterminus of DNP; it activates both GC-A and GC-B. Natriuretic peptides also bind to the non-GC-linked natriuretic peptide C receptor, the biological significance of which beyond NP clearance is currently unclear. Cyclic GMP modulates cGMP-dependent protein kinase G, cGMP-regulated PDEs, and cGMP-regulated cation channels. The cGMP signal is terminated by PDEs that hydrolyze cGMP to GMP, or by extrusion into the extracellular space. The NPs are degraded by a variety of peptidases. Cyclic GMP signaling can be enhanced by (1) the use of NO mimetics such as nitrovasodilators, (2) direct sGC stimulators, (3) exogenous NPs, (4) inhibiting NP degrading enzymes, and (5) inhibiting the activity of cGMP-hydrolyzing PDEs. ANP, atrial natriuretic peptide; BNP, B-type natriuretic peptide; cGMP, cyclic guanosine monophosphate; GMP, guanosine monophosphate; GC, guanylyl cyclase; DNP, Dendroaspis natriuretic peptide; DPP4, dipeptidyl peptidase IV; NEP, neutral endopeptidase; NO, nitric oxide; PDE, phosphodiesterase; PKG, protein kinase G; RA, natriuretic peptide receptor A; sGC, soluble guanylate cyclase.
Schematic illustrating three different forms of soluble guanylate cyclase and their respective responsiveness to nitrovasodilators, heme-dependent sGC stimulators (e.g., BAY 41-2272), and heme-independent sGC activators (e.g., cinaciguat [also known as BAY 58-2667]). Nitric oxide (NO) and nitrovasodilators only stimulate sGC when it, contains the heme moiety with a ferrous iron (Fe 2+); furthermore, NO and nitrovasodilators have cGMP-independent actions. BAY 41-2272 also activates only the NO-sensitive sGC but without the cGMP-independent actions of NO and nitrovasodilators. Cinaciguat activates heme-free sGC, which is insensitive to NO, and also inhibits its degradation. The question marks indicate that little is known about the transition between the different forms, their prevalence in health and disease, and their potential restoration to the reduced, NO-sensitive form. cGMP, cyclic guanosine monophosphate; Fe, iron; sGC, soluble guanylate cyclase. (From Boerrigter G, Burnett JC Jr. Soluble guanylate cyclase: not a dull enzyme. Circulation 2009;119(21):2752-2754.)
Mechanism of action of novel contractility-enhancing medications. Levosimendan enhances contractility by increasing responsiveness of myofilaments to calcium. The cardiac myosin activator CK 1827-452 stimulates myosin adenosine triphosphatase (ATPase), thereby increasing force generation. Istaroxime inhibits activity of plasma membrane sodium-potassium ATPase and increases the activity of sarcoplasmic/endoplasmic reticulum calcium ATPase (SERCA). ADP, adenosine diphosphate; ATP, adenosine triphosphate; I-1, protein phosphatase inhibitor-1; P, phosphate; PLB, phospholamban; PP1, protein phosphatase; RyR2, ryanodine receptor; TnC, troponin C; TnI, troponin I; TnT, troponin T. (Modified from Tavares M, Rezlan E, Vostroknoutova I, et al. New pharmacologic therapies for acute heart failure. Crit Care Med 2008; 36[Suppl]:S112-S120.)
Forrester Hemodynamic SubsetsSubset Description
I: Warm and dry (normal) PCWP 15–18 mmHg and CI >2.2 L/min/m2
II: Warm and wet (congestion) PCWP >18 mmHg and CI >2.2 L/min/m2
III: Cold and dry (hypoperfusion) PCWP 15–18 mmHg and CI <2.2 L/min/m2
IV: Cold and wet (congestion and hypoperfusion)
PCWP >18 mmHg and CI <2.2 L/min/m2
Treatment Goals for ADHF•Improve symptoms, especially congestion and low-output sympt.•Restore normal oxygenation•Optimize volume status•Identify etiology•Identify and address precipitating factors•Optimize chronic oral therapy•Minimize side effects•Identify patients who might benefit from revascularization•Identify patients who might benefit from device therapy•Identify risk of thromboembolism and need for anticoagulation•Educate patients concerning medications and self-management of heart failure•Consider and, where possible, initiate a disease-mgt. program
Subset I: Warm and Dry• Therapy is the optimization of oral medications
Pharmacotherapy for ADHF
Subset II: Warm and Wet• Patient has hypervolemia• IV diuretics and plus or minus vasodilators, nesiritide
Subset III: Cold and Dry• Patient has hypoperfusion• Therapy:
oIf PCWP <15 mmHg, IV fluids until PCWP 15–18 mmHgoIf PCWP ≥15 mmHg and MAP <50 mmHg, IV dobutamineoIf PCWP ≥15 mmHg, MAP ≥50 mmHg and compelling indication for inotrope, IV inotropeoIF PCWP ≥15 mmHg, MAP ≥50 mmHg and no compelling indication for inotrope, IV vasodilator
Pharmacotherapy for ADHF
Subset IV: Cold and Wet• Patient has hypoperfusion and hypervolemia• Therapy:
oIV diureticsoIf MAP <50 mmHg, IV dobutamineoIf MAP ≥50 mmHg and compelling indication for inotrope, IV inotropeoIf MAP ≥50 mmHg and no compelling indication for inotrope, IV vasodilator
Pharmacotherapy for ADHF
Discharge Criteria for Patients With ADHF•Treat exacerbating factors (i.e., discontinuation of contraindicated medications)Patient is at a "dry" weightOral medication regimen stable for 24 hoursPatient and family education completed, including clear discharge instructionsLeft ventricular ejection fraction documentedSmoking cessation counseling initiatedFollow-up clinic visit scheduled, 7 to 10 days outOptimal pharmacologic therapy achieved or intolerance documentedPlans for postdischarge management
Ideal properties for an acute heart failuresyndromes therapy
• Improve signs and symptoms (e.g. dyspnoea)• Improve haemodynamics without adversely effecting heart rate
and blood pressure• Improve the neurohumoral profile• Do not cause myocardial and/or kidney damage• Be effective in the context of current evidence-based therapy
such as ACE-I and beta-blockers• Demonstrate efficacy in both the acute and chronic setting• Be affordable• Reduce both in-hospital and post-discharge morbidity and
mortality.
Differential diagnosis include :
• Myocardial infarction• Congestive HF• Pneumonia• COPD exacerbation• Cardiac tamponade• Anxiety• Pulmonary embolism• Asthma
Medicine and dietary non compliance :
Cardiac causes•Ischemia•Arrhythmia•Uncontrolled hypertension
Noncardiac causes•Infection (pneumonia with or without hypoxia)•Exacerbation of comorbidity (chronic obstructive pulmonary disease)•Pulmonary embolus
Toxins (nonsteroidal anti-inflammatory drugs)Volume overload
Istaroxime: Na/K-ATPase Inhibitor
Change in left ventricular dP/dtmax comparing istaroxime (PST-2744) to dobutamine in 5 dogs with chronic ischemic heart failure. No difference was found between PST-2744 and 5 μg/kg/min dobutamine. Both significantly increased dP/dtmax (p < 0.05). Reproduced with permission.J Am Coll Cardiol. 2006;48(12):2397-2409.
Responses of Natriuretic Peptides, ET-1, and Cortisol
Mean 95% confidence interval of atrial natriuretic peptide (ANP), brain natriuretic peptide (BNP), cortisol, endothelin-1 (ET-1), and N-terminal pro-brain natriuretic peptide (NT-proBNP) during and after 4-h infusions (shaded in gray) of placebo (open circles) or urocortin (Ucn2) (solid circles). *p < 0.05 and **p < 0.01 indicate significant time-by-treatment interaction in the specific time phase.
Chan et al. JACC: Heart Failure Vol. 1, No. 5, 2013
Responses of Ucn-2, PRA, AngII, Aldosterone, andUcn-1
Mean 95% confidence interval of plasma aldosterone, angiotensin-II (AngII), plasma renin activity (PRA), urocortin-2 (Ucn2), and urocortin-1 (Ucn1) during and after 4-h infusions (shaded in gray) of placebo (open circles) or Ucn2 (solidcircles). yp < 0.001 indicates significant time-by-treatment interaction in the specific time phase.
Chan et al. JACC: Heart Failure Vol. 1, No. 5, 2013
Pulmonary Pressures, Cardiac Output, and Calculated
Total Peripheral Resistance Responses
Right heart catheter parameters (mean SEM) during and after 4-h infusions (shaded in gray) of placebo (open circles) or urocortin-2 (solid circles). *p < 0.05 and yp < 0.001 indicate significant time-by-treatment interaction in the specific time phase. cTPR ¼ calculated total peripheral resistance; PAP ¼ pulmonary artery pressure; PCWP ¼ pulmonary capillary wedge pressure; RA ¼ right atrial.
Chan et al. JACC: Heart Failure Vol. 1, No. 5, 2013
Congestion at rest
Low perfustion
at rest
No Yes Warm &
dry PCWP normal CI
normal
Warm & wet PCWP elevatedCI
normal
Cold & dry PCWP low / normal CI decreased
Cold & wet PCWP elevated CI decreased
Normal SVR High SVR
Natriuretic Peptides
Nesiritide
Or
Vasodilators Nitroprusside Nitroglycerine
No
Yes
Inotropic Drugs Dobutamine Milrinone
Calcium Sensitizers
Objective:•To evaluate the safety, pharmacokinetics/ pharmacodynamics, and efficacy of IV omecamtiv mecarbil (OM) in patients with acute heart failure (AHF)
Hypothesis: •At least 1 dose level of IV OM will be well tolerated and will result in improvement of dyspnoea in subjects with left ventricular systolic dysfunction hospitalised for AHF
ATOMIC-AHFAcute Treatment with Omecamtiv
Mecarbil to Increase Contractility in Acute Heart Failure
Randomised, double-blind, placebo-controlled,
sequential cohort study 1:1 randomizations Omecamtiv vs Placebo
Study Design: Sequential Dosing Cohort
Cohort 1 Cohort 2 Cohort 3Omecamtiv
Placebo1:1 Randomization (n≈200)
Omecamtiv
Placebo1:1 randomization (n≈200)
Placebo
Omecamtiv1:1 randomization (n≈200)
DMC DMC
Cohort 1 Cohort 2 Cohort 315 mg/hr @ 0-4 hr3 mg/hr @ 4-48 hr
Target: 230 ng/mLCmax: 75-500
ng/mLSET: ~8-55 msec
20 mg/hr @ 0-4 hr4 mg/hr @ 4-48 hrTarget: 310 ng/mL
Cmax: 125-700 ng/mL
SET: ~14-78 msec
7.5 mg/hr @ 0-4 hr1.5 mg/hr @ 4-48 hrTarget: 115 ng/mL
Cmax: 30-250 ng/mL SET: ~3-28 msec
Pharmacokinetic simulations
Teerlink JR, et al. Lancet 2011; 378: 667–75; Cleland JGF, et al. Lancet 2011; 378: 676–83.